PLoS Biology (Mar 2023)

An AI-guided screen identifies probucol as an enhancer of mitophagy through modulation of lipid droplets

  • Natalia Moskal,
  • Naomi P. Visanji,
  • Olena Gorbenko,
  • Vijay Narasimhan,
  • Hannah Tyrrell,
  • Jess Nash,
  • Peter N. Lewis,
  • G. Angus McQuibban

Journal volume & issue
Vol. 21, no. 3

Abstract

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Failures in mitophagy, a process by which damaged mitochondria are cleared, results in neurodegeneration, while enhancing mitophagy promotes the survival of dopaminergic neurons. Using an artificial intelligence platform, we employed a natural language processing approach to evaluate the semantic similarity of candidate molecules to a set of well-established mitophagy enhancers. Top candidates were screened in a cell-based mitochondrial clearance assay. Probucol, a lipid-lowering drug, was validated across several orthogonal mitophagy assays. In vivo, probucol improved survival, locomotor function, and dopaminergic neuron loss in zebrafish and fly models of mitochondrial damage. Probucol functioned independently of PINK1/Parkin, but its effects on mitophagy and in vivo depended on ABCA1, which negatively regulated mitophagy following mitochondrial damage. Autophagosome and lysosomal markers were elevated by probucol treatment in addition to increased contact between lipid droplets (LDs) and mitochondria. Conversely, LD expansion, which occurs following mitochondrial damage, was suppressed by probucol and probucol-mediated mitophagy enhancement required LDs. Probucol-mediated LD dynamics changes may prime the cell for a more efficient mitophagic response to mitochondrial damage. Failures in mitophagy, a process by which damaged mitochondria are cleared, results in neurodegeneration, while enhancing mitophagy promotes the survival of dopaminergic neurons. This study shows that the effects of Probucol on lipid droplet expansion can augment mitophagy in neurons, leading to locomotor improvements in zebrafish and fly models of Parkinson’s disease.